The biogenesis of new polypeptides by ribosomes and their subsequent correct folding and localization to the appropriate cellular compartments are essential key processes to maintain protein homoeostasis. These complex mechanisms are governed by a repertoire of protein biogenesis factors that directly bind to the ribosome and chaperone nascent polypeptide chains as soon as they emerge from the ribosomal tunnel exit. This nascent chain ‘welcoming committee’ regulates multiple co-translational processes including protein modifications, folding, targeting and degradation. Acting at the front of the protein production line, these ribosome-associated protein biogenesis factors lead the way in the cellular proteostasis network to ensure proteome integrity. In this article, I focus on three different systems in eukaryotes that are critical for the maintenance of protein homoeostasis by controlling the birth, life and death of nascent polypeptide chains.
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October 2016
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Patricija van Oosten-Hawle
Patricija van Oosten-Hawle
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A schematic depiction of protease network in mitochondria. In this issue, Voos et al. review mitochondrial protein quality control, looking at the biochemical processes and the enzymatic components that are responsible for maintaining mitochondrial protein homeostasis; see pages 213–225. - PDF Icon PDF LinkTable of Contents
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Review Article|
October 15 2016
Protein quality control at the ribosome: focus on RAC, NAC and RQC
Martin Gamerdinger
1Department of Biology, Institute of Molecular Microbiology, University of Konstanz, 78457 Konstanz, Germany
Correspondence: Martin Gamerdinger (email martin.gamerdinger@uni-konstanz.de).
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Essays Biochem (2016) 60 (2): 203–212.
Article history
Received:
January 14 2016
Revision Received:
April 16 2016
Accepted:
May 09 2016
Citation
Patricija van Oosten-Hawle, Martin Gamerdinger; Protein quality control at the ribosome: focus on RAC, NAC and RQC. Essays Biochem 15 October 2016; 60 (2): 203–212. doi: https://doi.org/10.1042/EBC20160011
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